Generation of a novel mouse strain with conditional, cell-type specific, expression of DND1

Lisa Nunez; Sharada Mokkapati; Chengtai Yu; Jian M. Deng; Richard R. Behringer; Angabin Matin

doi:10.1002/dvg.23335

Generation of a novel mouse strain with conditional, cell-type specific, expression of DND1

Lisa Nunez, Sharada Mokkapati, Chengtai Yu, Jian M. Deng, Richard R. Behringer, Angabin Matin

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

Dead-End 1 (DND1) encodes an RNA binding protein critical for viable primordial germ cells in vertebrates. When introduced into cancer cell lines, DND1 suppresses cell proliferation and enhances apoptosis. However, the molecular function of mammalian wild-type DND1 has mostly been studied in cell lines and not verified in the organism. To facilitate study of wild-type DND1 function in mammalian systems, we generated a novel transgenic mouse line, LSL-FM-DND1^flox/+, which conditionally expresses genetically engineered, FLAG-tagged and myc-tagged DND1 in a cell type-specific manner. We report that FLAG-myc-DND1 is indeed expressed in specific tissues of the mouse when LSL-FM-DND1^flox/+ is combined with mouse strains expressing Cre-recombinase. LSL-FM-DND1^flox/+ mice are fertile with no overt health effects. We expressed FLAG-myc-DND1 in the pancreas and found that chronic, ectopic expression of FLAG-myc-DND1 led to increase in fasting glucose levels in older mice. Thus, this novel LSL-FM-DND1^flox/+ mouse strain will facilitate studies on the biological and molecular function of wild-type DND1.

Original language	English (US)
Article number	e23335
Journal	Genesis
Volume	57
Issue number	11-12
DOIs	https://doi.org/10.1002/dvg.23335
State	Published - Nov 1 2019

Keywords

FLAG-myc-DND1
conditional
transgenic LSL-FM-DND1 mice

ASJC Scopus subject areas

Genetics
Endocrinology
Cell Biology

MD Anderson CCSG core facilities

Genetically Engineered Mouse Facility
Research Animal Support Facility

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10.1002/dvg.23335

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title = "Generation of a novel mouse strain with conditional, cell-type specific, expression of DND1",

abstract = "Dead-End 1 (DND1) encodes an RNA binding protein critical for viable primordial germ cells in vertebrates. When introduced into cancer cell lines, DND1 suppresses cell proliferation and enhances apoptosis. However, the molecular function of mammalian wild-type DND1 has mostly been studied in cell lines and not verified in the organism. To facilitate study of wild-type DND1 function in mammalian systems, we generated a novel transgenic mouse line, LSL-FM-DND1flox/+, which conditionally expresses genetically engineered, FLAG-tagged and myc-tagged DND1 in a cell type-specific manner. We report that FLAG-myc-DND1 is indeed expressed in specific tissues of the mouse when LSL-FM-DND1flox/+ is combined with mouse strains expressing Cre-recombinase. LSL-FM-DND1flox/+ mice are fertile with no overt health effects. We expressed FLAG-myc-DND1 in the pancreas and found that chronic, ectopic expression of FLAG-myc-DND1 led to increase in fasting glucose levels in older mice. Thus, this novel LSL-FM-DND1flox/+ mouse strain will facilitate studies on the biological and molecular function of wild-type DND1.",

keywords = "FLAG-myc-DND1, conditional, transgenic LSL-FM-DND1 mice",

author = "Lisa Nunez and Sharada Mokkapati and Chengtai Yu and Deng, {Jian M.} and Behringer, {Richard R.} and Angabin Matin",

note = "Funding Information: This work was funded by NCI R21CA175833. We acknowledge use of Molecular Biology research infrastructure support from NIMHD 5G12MD007605 and Genetically Engineered Mouse Facility at MD Anderson Cancer Center NCI CA016672 (GEMF). We thank M.-J. Tsai for the shuttle vector, P. Chiao for Pdx-1-Cre mice, A. Shivachar, P. Ogounu, J.D. Godavarthi, and R. Zhang for technical assistance. Publisher Copyright: {\textcopyright} 2019 Wiley Periodicals, Inc.",

year = "2019",

month = nov,

day = "1",

doi = "10.1002/dvg.23335",

language = "English (US)",

volume = "57",

journal = "Genesis",

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AU - Nunez, Lisa

AU - Mokkapati, Sharada

AU - Yu, Chengtai

AU - Deng, Jian M.

AU - Behringer, Richard R.

AU - Matin, Angabin

N1 - Funding Information: This work was funded by NCI R21CA175833. We acknowledge use of Molecular Biology research infrastructure support from NIMHD 5G12MD007605 and Genetically Engineered Mouse Facility at MD Anderson Cancer Center NCI CA016672 (GEMF). We thank M.-J. Tsai for the shuttle vector, P. Chiao for Pdx-1-Cre mice, A. Shivachar, P. Ogounu, J.D. Godavarthi, and R. Zhang for technical assistance. Publisher Copyright: © 2019 Wiley Periodicals, Inc.

PY - 2019/11/1

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N2 - Dead-End 1 (DND1) encodes an RNA binding protein critical for viable primordial germ cells in vertebrates. When introduced into cancer cell lines, DND1 suppresses cell proliferation and enhances apoptosis. However, the molecular function of mammalian wild-type DND1 has mostly been studied in cell lines and not verified in the organism. To facilitate study of wild-type DND1 function in mammalian systems, we generated a novel transgenic mouse line, LSL-FM-DND1flox/+, which conditionally expresses genetically engineered, FLAG-tagged and myc-tagged DND1 in a cell type-specific manner. We report that FLAG-myc-DND1 is indeed expressed in specific tissues of the mouse when LSL-FM-DND1flox/+ is combined with mouse strains expressing Cre-recombinase. LSL-FM-DND1flox/+ mice are fertile with no overt health effects. We expressed FLAG-myc-DND1 in the pancreas and found that chronic, ectopic expression of FLAG-myc-DND1 led to increase in fasting glucose levels in older mice. Thus, this novel LSL-FM-DND1flox/+ mouse strain will facilitate studies on the biological and molecular function of wild-type DND1.

AB - Dead-End 1 (DND1) encodes an RNA binding protein critical for viable primordial germ cells in vertebrates. When introduced into cancer cell lines, DND1 suppresses cell proliferation and enhances apoptosis. However, the molecular function of mammalian wild-type DND1 has mostly been studied in cell lines and not verified in the organism. To facilitate study of wild-type DND1 function in mammalian systems, we generated a novel transgenic mouse line, LSL-FM-DND1flox/+, which conditionally expresses genetically engineered, FLAG-tagged and myc-tagged DND1 in a cell type-specific manner. We report that FLAG-myc-DND1 is indeed expressed in specific tissues of the mouse when LSL-FM-DND1flox/+ is combined with mouse strains expressing Cre-recombinase. LSL-FM-DND1flox/+ mice are fertile with no overt health effects. We expressed FLAG-myc-DND1 in the pancreas and found that chronic, ectopic expression of FLAG-myc-DND1 led to increase in fasting glucose levels in older mice. Thus, this novel LSL-FM-DND1flox/+ mouse strain will facilitate studies on the biological and molecular function of wild-type DND1.

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Generation of a novel mouse strain with conditional, cell-type specific, expression of DND1

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

Access to Document

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